Integrin-mediated survival signals regulate the apoptotic function of Bax through its conformation and subcellular localization

Andrew P. Gilmore, Anthony D. Metcalfe, Lewis H. Romer, Charles H. Streuli

    Research output: Contribution to journalArticlepeer-review

    Abstract

    Most normal cells require adhesion to extracellular matrix for survival, but the molecular mechanisms that link cell surface adhesion events to the intracellular apoptotic machinery are not understood. Bcl-2 family proteins regulate apoptosis induced by a variety of cellular insults through acting on internal membranes. A pro-apoptotic Bcl-2 family protein, Bax, is largely present in the cytosol of many cells, but redistributes to mitochondria after treatment with apoptosis-inducing drugs. Using mammary epithelial cells as a model for adhesion-regulated survival, we show that detachment from extracellular matrix induced a rapid translocation of Bax to mitochondria concurrent with a conformational change resulting in the exposure of its BH3 domain. Bax translocation and BH3 epitope exposure were reversible and occurred before caspase activation and apoptosis. Pp125FAK regulated the conformation of the Bax BH3 epitope, and PI 3-kinase and pp60src prevented apoptosis induced by defective pp125FAK signaling. Our results provide a mechanistic connection between integrin-mediated adhesion and apoptosis, through the kinase-regulated subcellular distribution of Bax.
    Original languageEnglish
    Pages (from-to)431-445
    Number of pages14
    JournalJournal of Cell Biology
    Volume149
    Issue number2
    DOIs
    Publication statusPublished - 17 Apr 2000

    Keywords

    • Adhesion
    • Apoptosis
    • Bax
    • Mammary
    • pp125FAK

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